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力达霉素作用下膀胱癌细胞与小牛胸腺DNA相互作用行为的分子动力学及多光谱研究:通过下调PI3K/AKT信号通路诱导细胞凋亡

Molecular Dynamics and Multi-Spectroscopic of the Interaction Behavior between Bladder Cancer Cells and Calf Thymus DNA with Rebeccamycin: Apoptosis through the Down Regulation of PI3K/AKT Signaling Pathway.

作者信息

Malek-Esfandiari Zohreh, Rezvani-Noghani Azadeh, Sohrabi Tahmineh, Mokaberi Parisa, Amiri-Tehranizadeh Zeinab, Chamani Jamshidkhan

机构信息

Department of Biology, Faculty of Sciences, Mashhad Branch, Islamic Azad University, Mashhad, Iran.

Medical Chemistry Department, School of Pharmacy, Mashhad University of Medical Sciences, Mashhad, Iran.

出版信息

J Fluoresc. 2023 Jul;33(4):1537-1557. doi: 10.1007/s10895-023-03169-4. Epub 2023 Feb 14.

Abstract

The interaction of Rebeccamycin with calf thymus (ctDNA) in the absence and presence of H1 was investigated by molecular dynamics, multi-spectroscopic, and cellular techniques. According to fluorescence and circular dichroism spectroscopies, Rebeccamycin interacted with ctDNA in the absence of H1 through intercalator or binding modes, while the presence of H1 resulted in revealing theintercalator, as the dominant role, and groove binding modes of ctDNA-Rebeccamycin complex. The binding constants, which were calculated to be 1.22 × 10 M and 7.92 × 10 M in the absence and presence of H1, respectively, denoted the strong binding of Rebeccamycin with ctDNA. The binding constants of Rebeccamycin with ct DNA in the absence and presence of H1 were calculated at 298, 303 and 308 K. Considering the thermodynamic parameters (ΔH and ΔS), both vander waals forces and hydrogen bonds played predominant roles throughout the binding of Rebeccamycin to ctDNA in the absence and presence of H1. The outcomes of circular dichroism suggested the lack of any major conformational changes in ctDNA upon interacting with Rebeccamycin, except some perturbations in native B-DNA at local level. Additionally, the effect of NaCl and KI on ctDNA-Rebeccamycin complex provided further evidence for the reliance of their interaction modes on substituted groups. The observed increase in the relative viscosity of ctDNA caused by the enhancement of Rebeccamycin confirmed their intercalation and groove binding modes in the absence and presence of H1. Moreover, the assessments of molecular docking simulation corroborated these experimental results and also elucidated the effectiveness of Rebeccamycinin inhibiting and proliferating T24 and 5637 cells. Meanwhile, the ability of Rebeccamycin in inhibiting cell proliferation and tumor growth through the induction of apoptosis by down regulating the PI3K/AKT signaling pathway were provided.

摘要

通过分子动力学、多光谱和细胞技术研究了瑞贝卡霉素在不存在和存在H1的情况下与小牛胸腺(ctDNA)的相互作用。根据荧光和圆二色光谱,瑞贝卡霉素在不存在H1的情况下通过嵌入或结合模式与ctDNA相互作用,而H1的存在导致揭示出嵌入作用作为主要作用以及ctDNA-瑞贝卡霉素复合物的沟槽结合模式。在不存在和存在H1的情况下计算得到的结合常数分别为1.22×10⁶ M和7.92×10⁶ M,表明瑞贝卡霉素与ctDNA有强结合。在298、303和308 K下计算了瑞贝卡霉素在不存在和存在H1时与ctDNA的结合常数。考虑到热力学参数(ΔH和ΔS),范德华力和氢键在瑞贝卡霉素在不存在和存在H1时与ctDNA的结合过程中都起主要作用。圆二色性的结果表明,ctDNA与瑞贝卡霉素相互作用后除了在局部水平上对天然B-DNA有一些扰动外,没有任何主要的构象变化。此外,NaCl和KI对ctDNA-瑞贝卡霉素复合物的影响为它们的相互作用模式对取代基团的依赖性提供了进一步的证据。瑞贝卡霉素浓度增加导致ctDNA相对粘度增加,证实了它们在不存在和存在H1时的嵌入和沟槽结合模式。此外,分子对接模拟评估证实了这些实验结果,还阐明了瑞贝卡霉素抑制和增殖T24和5637细胞的有效性。同时,还提供了瑞贝卡霉素通过下调PI3K/AKT信号通路诱导凋亡来抑制细胞增殖和肿瘤生长的能力。

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